DCVMN Annual General Meeting · ICH - Quality of Biotechnological Products: Stability Testing of...
Transcript of DCVMN Annual General Meeting · ICH - Quality of Biotechnological Products: Stability Testing of...
Bernardo Luiz Moraes Moreira
Second Board – Assessor
ANVISA
Rio de Janeiro, 2019
Vaccine Regulatory Framework and Agency Modernization
DCVMN Annual General Meeting
➢ Biological Products
➢Vaccines;
➢Hyperimmune sera;
➢Blood products;
➢Biomedicines classified as:
a) medicines obtained from biological fluids or animal-originated tissue; b) medicines obtained through biotechnological procedures.
➢Medicines containing live, attenuated or dead microorganisms;
➢Probiotics;
➢Allergens.2
RDC 55/2010 Marketing Authorization
RDC 46/2000 Blood products
RDC 323/2003 Probiotics
RDC 50/2011 Stability
RDC 47/2009 Package insert
RDC 71/2009 Labelling
RDC 301/2019 GMP
RDC 194/2017 Allergenics
RDC 187/2017 Hyperimmune Sera
Law 6.360/1976 Decree 8.077/2013
RDC 234/2005 Quality control
RDC 49/2011 Post-approval
changes
3
Regulatory framework
4
Regulatory framework
New Biological Product: biological product containing a drug substance with a known biologic activity not yet licensed in Brazil ! innovator product ! reference product
(Non new) Biological Product: biological product containing a drug substance with a known biologic activity already licensed in Brazil.
RDC n° 55/2010
❖ Resolution RDC 55/2010
Marketing authorization of Biological Products in Brazil
Biosimilars
Regulatory framework
Stand alone approach
5
Vaccines – General Requirements
➢ Immunobiological medicines containing one or more antigens, when innoculated are able to induce active and specific immunity in order to protect, reduce the severity or fight the diseases caused by the microorganism.
➢ GMP for all manufacturers issued by Anvisa.
➢ CMC Report
➢ Clinical Data Report
➢ Pharmacovigilance Report
➢ Package insert and label draft
Vaccines – CMC Report
➢ Description of manufacturers (cell bank, drug substance, intermediates, drug product)
➢ History of product development
➢ Manufacturing (manufacturing summary, IPC, equipments, critical steps, batch size, validation report for critical steps)
➢ Quality Control ( tests and specifications DS – DP, analythical method validation, reference standards)
➢ Transport validation
➢ Excipients (QC tests and specifications, preservative efficacy, physical-chemical interaction with API)
➢ Stability protocol and report
➢ Impurities characterization and specification; adventitious agents evaluation for starting materials
Vaccines – Specific Requirements
➢ Strains – origin, identification, atenuation process, certificate of analysis.
➢ Master and working seed lot – origin, identification, characterization, stability, adventitious agents.
➢ Master and working cell banks – beside MSL and WSL requirements, passage number definition.
➢ Embryonated eggs – origin, identification and certificate of analysis.
➢ Maximum in vitro age determination.
➢ Manufacturing process and Quality control of carrier protein.
➢ Description of conjugation and inativation process.
Pre-submission Meeting
Electronic or manual submission
Individual review External expert
Final opinion and decision letter
Applicant’s response List of questions
Review process for market authorization
❖ Resolution RDC 49/2011 Stablishes requirements and procedures for post-approval changes of Biological Products
❖ Resolution RDC 50/2011 Stablishes requirements and procedures for stability studies of Biological Products
Post-approval changes and stability
Under review
10
11
Resolution on Stability (RDC 50/2011)
✓ Objectives:
• Update the procedures and conditions for conducting stability studies of biological products;
• Alignment with Q5C principles and other complementary guidelines.
12
✓ References: ❖ ICH - Quality of Biotechnological Products: Stability Testing of Biotechnological/
Biological Products - Q5C • ICH - Stability testing of new drug substances and products - Q1A(R2);
• ICH - Stability testing: photostability testing of new drug substances and products – Q1B; • ICH - Bracketing and matrixing designs for stability testing of new drug substances and products
- Q1D; • ICH - Specifications: test procedures and acceptance criteria for biotechnological/biological
products - Q6B; • ICH - Validation of analytical procedures: text and methodology - Q2(R1); • CPMP - Note for guidance on in-use stability testing of human medicinal products.
Resolution on Stability (RDC 50/2011)
13
Resolution on Stability (RDC 50/2011)
✓ Main topics • Stability protocol; • Long term stability (conditions); • Accelerated/stress stability (conditions); • Photostability (conditions); • Cycling studies (conditions); • In use stability; • Stability requirements for marketing authorization application (DS, intermediates,
diluents, adjuvants, reference standards, DP).
* Stability for post-approval
14
Resolution on Post-approval changes
✓ Objectives:
• Update procedures, data requirements and categorization for post-approval changes of biological products of RDC 49/2011;
• Alignment with WHO guideline for changes to approved biotherapeutic products and other complementary guidelines.
15
✓ Main references:
• Guidelines on procedures and data requirements for changes to approved biotherapeutic products – WHO 2017;
• Guidelines on procedures and data requirements for changes to approved vaccines - Annex 4 WHO Technical Report Series No. 993, 2015;
• Guidance Document Post-Notice of Compliance (NOC) Changes: Quality Document - Appendix 3: Quality Post-NOC Changes (Biologics), Health Canada 2016;
• Guidance Document Post-Notice of Compliance (NOC) Changes: Safety and Efficacy Document, Health Canada 2018.
Resolution on Post-approval changes
16
✓ Main topics
• Quality changes: refer to CMC changes (manufacturing process, quality control testing, equipment, facility, product composition, stability)
❑ Drug Substance (manufacture, control, reference standards, container closure system, stability)
❑ Drug Product (description and composition, diluent, adjuvant ,manufacture, control, reference standards, container closure system, stability)
Resolution on Post-approval changes
17
✓ Main topics
• Safety and Efficacy and Labelling changes:
Refer to changes that have an impact on the clinical use of the biological product (e.g., addition or expansion of a safety or efficacy claim, including expansion of the population; change in the route of administration; change in the recommended dose/dosing range; co-administration with other biotherapeutic products or medicines; changes that have the potential to improve the risk management measures (e.g., new adverse events, instructions on dosing, deletion or reduction of contraindications).
Resolution on Post-approval changes
Prioritization
Resolution RDC nº 204, December 27th, 2017
• Focus on prioritizing drug registrations relevant to public health • Highlights:
• Pediatric population; • Neglected diseases; • Emerging or reemerging diseases; • Public Health Emergencies; • Serious debilitating conditions; • Vaccines to be incorporated in the National Immunization Program; • First 3 new generics for a given drug.
Prioritization
Resolution RDC nº 204, December 27th, 2017
• Focus on prioritizing post-approval changes for: • Rare diseases; • Pediatric population; • Neglected diseases; • Emerging or reemerging diseases; • Public Health Emergencies; • Serious debilitating conditions; • Vaccines to be incorporated in the National Immunization
Program.
Resolution RDC nº 204, December 27th, 2017
• Timelines for the final decision:
• 120 days - registration (365 days for ordinary category); • 60 days - post-approval changes (180 days for ordinary category);
• 45 days - clinical trial submissions (90 days for ordinary category)
Prioritization
Resolution RDC nº 205, December 28th, 2017 ✓Establishes special procedures for clinical trials, GMP certification and registration of new drugs.
✓Applies to medicines for rare diseases used in serious debilitating conditions and proposed to
change in a clinically significant way the evolution of the disease or make possible the remission
of the disease.
Drugs for Rare Diseases
Resolution RDC nº 205, December 28th, 2017 ✓Faster procedures;
✓Differentiated criteria compared to conventional procedures, but not compromising safety,
efficacy and quality (eg. CTD format, suppression of quality control in Brazil, ongoing stability
studies, ongoing phase III clinical trials);
✓Stimulate the conduction of clinical trials and the license of medicines for rare diseases.
Drugs for Rare Diseases
RDC nº 205/2017 - timelines
Drugs for Rare Diseases
Clinical Trial Consent Anvisa: 30 days for first analysis
Company: 30 days for reply Anvisa: 30 days for analysis of
response
Registration Anvisa: 60 days for first analysis
Company: 30 days for reply Anvisa: 45 days for analysis of
response
Pricing
Company: protocol concomitant with the registration request
Commercialization
Company: 365 days after publication of the registration
Certificate of Good Manufacturing Pratices
Anvisa: 120 days for publishing the decision
Registrations granted
0
225
450
675
900
2014 2015 2016 2017 2018
➢ I n 2 0 1 8 , A n v i s a h a d a u t h o r i z e d 8 2 7 d r u g registrations.
➢ 1 7 3 p r i o r i zat i o n s we re granted.
➢ 10 new medicines for rare diseases.
Timelines for registration of prioritized drugs in 2018
Prioritized Biologicals
45
134
21
Backlog time Anvisa time Company time
Prioritized New Synthetic
110
210
61
Backlog time Anvisa time Company time
OS Nº 45, February 2018 (Service Orientation)
➢Establishes a Optimized Review Pathway for Biological Products (registration and variations/post approval changes);
➢Elegibily criteria: Registered in the USFDA and EMA; same indications; dosage; adverse reactions; precautions.
➢Approval Reports should be provided
Reliance Projects
• Drug Approval and Refusal Letters
✓ Make drug letters available on Anvisa’s website.
✓ Anvisa’s reasons to approve or refuse a product.
Transparency
29
Search for the information available on Anvisa’s website
Product’s prescribing information http://portal.anvisa.gov.br/bulario-eletronico1
Authorized drugs http://portal.anvisa.gov.br/medicamentos/consultas
Public assessment reports http://www.anvisa.gov.br/datavisa/Fila_de_analise/index.asp
Clinical trials authorized http://www7.anvisa.gov.br/Datavisa/Consulta_Comunicados/Consulta_CE_Autorizados.asp
Anvisa’s legislation http://portal.anvisa.gov.br/legislacao#/
Regulatory agenda 2017-2020 http://portal.anvisa.gov.br/2017-2020
Transparency
Perspectives
• License of less complexity biological products;
• Review of resolutions for stability studies and post-approval changes of biological products;
• Timelines for license renew;
• Stability studies for synthetics;
• Implementation of the common technical document (CTD) for medicines registration.
• Implementation of Quality System for Biological Products in accordance with Good Revision Practices;
Transparência
Convergência regulatória
Responsabilidade compartilhada
PrevisibilidadeRacional técnico e científico
Goals
Transparency
Predictability
Shared responsibility
Regulatory convergence
Scientific and technical rational ANVISA
Thank you [email protected]
Agência Nacional de Vigilância Sanitária - Anvisa
SIA Trecho 5 - Área especial 57 - Lote 200
CEP: 71205-050
Brasília - DF
www.anvisa.gov.br
www.twitter.com/anvisa_oficial
Anvisa Atende: 0800-642-9782
http://portal.anvisa.gov.br/english